Thomas Peppard scite author profile

High‐dose betamethasone and dexamethasone are standard of care treatments for women at risk of preterm delivery to improve neonatal respiratory and mortality outcomes. The dose in current use has never been evaluated to minimize exposures while assuring efficacy. We report the pharmacokinetics and pharmacodynamics (PDs) of oral and intramuscular treatments with single 6 mg doses of dexamethasone phosphate, betamethasone phosphate, or a 1:1 mixture of betamethasone phosphate and betamethasone acetate in reproductive age South Asian women. Intramuscular or oral betamethasone has a terminal half‐life of 11 hours, about twice as long as the 5.5 hours for oral and intramuscular dexamethasone. The 1:1 mixture of betamethasone phosphate and betamethasone acetate shows an immediate release of betamethasone followed by a slow release where plasma betamethasone can be measured out to 14 days after the single dose administration, likely from a depo formed at the injection site by the acetate. PD responses were: increased glucose, suppressed cortisol, increased neutrophils, and suppressed basophils, CD3CD4 and CD3CD8 lymphocytes. PD responses were comparable for betamethasone and dexamethasone, but with longer times to return to baseline for betamethasone. The 1:1 mixture of betamethasone phosphate and betamethasone acetate caused much longer adrenal suppression because of the slow release. These results will guide the development of better treatment strategies to minimize fetal and maternal drug exposures for women at risk of preterm delivery.

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Quantitative 18F-FDG PET-CT scan characteristics correlate with tuberculosis treatment response

Malherbe

Chen

Dupont

et al. 2020

EJNMMI Res

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Background: There is a growing interest in the use of F-18 FDG PET-CT to monitor tuberculosis (TB) treatment response. Tuberculosis lung lesions are often complex and diffuse, with dynamic changes during treatment and persisting metabolic activity after apparent clinical cure. This poses a challenge in quantifying scan-based markers of burden of disease and disease activity. We used semi-automated, whole lung quantification of lung lesions to analyse serial FDG PET-CT scans from the Catalysis TB Treatment Response Cohort to identify characteristics that best correlated with clinical and microbiological outcomes.Results: Quantified scan metrics were already associated with clinical outcomes at diagnosis and 1 month after treatment, with further improved accuracy to differentiate clinical outcomes after standard treatment duration (month 6). A high cavity volume showed the strongest association with a risk of treatment failure (AUC 0.81 to predict failure at diagnosis), while a suboptimal reduction of the total glycolytic activity in lung lesions during treatment had the strongest association with recurrent disease (AUC 0.8 to predict pooled unfavourable outcomes). During the first year after TB treatment lesion burden reduced; but for many patients, there were continued dynamic changes of individual lesions. Conclusions: Quantification of FDG PET-CT images better characterised TB treatment outcomes than qualitative scan patterns and robustly measured the burden of disease. In future, validated metrics may be used to stratify patients and help evaluate the effectiveness of TB treatment modalities.

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Study of Aldosterone Synthase Inhibition as an Add‐On Therapy in Resistant Hypertension

Karns

Bral

Hartman³

et al. 2012

J of Clinical Hypertension

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Aldosterone inhibition with mineralcorticoid receptor antagonists (MRAs) is an effective treatment for resistant hypertension. Aldosterone synthase inhibitors (ASIs) are currently being investigated as a new therapeutic strategy to reduce aldosterone secretion from the adrenal gland. In this study, the efficacy and safety of the first-generation ASI LCI699 (0.25 mg twice daily, 1 mg 4 once daily, and 0.5 mg ⁄ 1 mg twice daily) was compared with placebo and eplerenone (50 mg twice daily), in patients with resistant hypertension. Placebo-adjusted decreases in systolic blood pressure (BP) with LCI699 ranged from 2.6 mm Hg to 4.3 mm Hg at week 8; changes in diastolic BP ranged from +0.3 mm Hg to )1.2 mm Hg. However, reductions were smaller than observed with eplerenone 50 mg twice daily (9.9 mm Hg and 2.9 mm Hg for systolic and diastolic BP, respectively) and not statistically significant vs placebo. LCI699 suppressed plasma aldosterone levels in a dose-related manner with corresponding dose-dependent increases in plasma renin activity and plasma 11-deoxycorticosterone. LCI699 and eplerenone were well tolerated. These data demonstrate that aldosterone synthesis inhibition with LCI699 lowers BP modestly in patients with resistant hypertension. Aldosterone synthesis inhibition might offer an attractive adjunct to aldosterone receptor blockade, although the potential of a combination MRA ⁄ ASI has not yet been tested. J Clin Hypertens (Greenwich). 2013; 15:186-192. Ó2012 Wiley Periodicals, Inc.Aldosterone plays an important role in blood pressure (BP) control and maintaining potassium and sodium homeostasis and in the pathophysiology of cardiovascular and renal disease.1-4 A relative aldosterone excess predicts hypertension onset 5 and aldosterone is believed to play a critical role in mediating and aggravating resistant hypertension, 6 a common clinical problem that affects 20% to 28% of patients with hypertension. 7,8 It was previously thought that primary aldosteronism is present in <1% of unselected hypertensive patients, but more recent estimates suggest that it affects closer to 10%, and these patients tend to have higher incidences of cardiovascular (CV) damage when controlled for sex, age, and BP status. Thus, aldosterone blockade represents an attractive therapeutic approach to lower BP and to reduce the risk of CV events and end-organ damage.One approach for blocking the effects of aldosterone is to prevent its binding to mineralocorticoid receptors, and two mineralocorticoid receptor antagonists (MRAs), eplerenone and spironolactone, have been shown to be effective for the treatment of hypertension and heart failure.10-14 A reduction in BP with spironolactone was associated with reduction in cardiac mass and improvement in diastolic function in patients with resistant hypertension. 15 However, MRAs induce a counter-regulatory increase in aldosterone concentration, which may limit the efficacy of mineralocorticoid receptor (MR) blockade by stimulating MR-independent effects of aldosterone. 16 Indeed, aldoste...

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Thomas Peppard

Pharmacokinetics and Pharmacodynamics of Intramuscular and Oral Betamethasone and Dexamethasone in Reproductive Age Women in India

Quantitative 18F-FDG PET-CT scan characteristics correlate with tuberculosis treatment response

Study of Aldosterone Synthase Inhibition as an Add‐On Therapy in Resistant Hypertension

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